All
All

What are you looking for?

All
Results
Organizations

Quick search

  • Projects supported by TA ČR
  • Excellent projects
  • Projects with the highest public support
  • Current projects

Smart search

  • That is how I find a specific +word
  • That is how I leave the -word out of the results
  • “That is how I can find the whole phrase”
EN
ČeštinaEnglish

Interfacial properties of alpha-synuclein and aggregation of this protein in Parkinson's disease

Project goals

Parkinson's disease is the second most common neurodegenerative disease that affects coordination of movement in sufferers, associated with the formation and deposition of amyloid fibrils of the protein alpha-synuclein (AS). Studies of AS aggregation invitro are associated with hopes for better understanding, diagnosing and therapy of the Parkinson's disease. It has been proposed that oligomeric intermediates on the pathway to fibrilization rather than the fibrils themselves are the pathogenic agents of Parkinson's disease, but efficient methods for their detection are lacking. Our recent results suggested that electrochemical methods may be useful in the research of AS aggregation and particularly of formation of the oligomeric intermediates. We wishto combine our experience in electrochemistry with other methods such as solid state NMR, fluorescence, atomic force microscopy or electron microscopy, available in the partner's lab to contribute to the progress in the field

Keywords

Electrochemistry of proteinsalpha-synuclein preagregation and aggregationCatalytic hydrogen evolutionMercury and carbon electrodesParkinson's disease

Public support

  • Provider

    Academy of Sciences of the Czech Republic

  • Programme

    The research grant projects for juniors

  • Call for proposals

    Juniorské badatelské grantové projekty 7 (SAV02009-B)

  • Main participants

  • Contest type

    VS - Public tender

  • Contract ID

    KJB100040901

Alternative language

  • Project name in Czech

    Mezifázové vlastnosti alfa-synucleinu a agregace tohoto proteinu v Parkinsonově nemoci

  • Annotation in Czech

    Parkinsonova nemoc je druhé nejčastější neurodegenerativní onemocnění ovlivňující koordinaci pohybů postiženého, spojované s tvorbou a ukládáním amyloidních fibril alfa-synucleinu (AS). Studium agregace AS in vitro je spojeno s očekáváním zlepšení poznatků o Parkinsonově nemoci, s následním využitím v diagnostice a terapii. Předpokládá se, že patogenním činitelem v Parkinsonově nemoci nejsou fibrily, ale oligomerní meziprodukty vznikající v procesu fibrilizace. Efektivní metoda pro detekci těchto oligomerních meziproduktů doposud chybí. Naše současné výsledky ukazují, že elektrochemické metody mohou být užitečné ve výzkumu agregace AS, obzvláště ve formování oligomerních meziproduktů. Chtěli bychom kombinovat naše zkušenosti v elektrochemii se zkušenostmi partnerských laboratoří v jiných metodách jako jsou NMR, fluorescence, atomová silová mikroskopie, elektronová mikroskopie, a tím přispět k dalšímu vývoji v této oblasti.

Scientific branches

  • R&D category

    ZV - Basic research

  • CEP classification - main branch

    BO - Biophysics

  • CEP - secondary branch

    CG - Electrochemistry

  • CEP - another secondary branch

    EB - Genetics and molecular biology

  • 10405 - Electrochemistry (dry cells, batteries, fuel cells, corrosion metals, electrolysis)
    10603 - Genetics and heredity (medical genetics to be 3)
    10604 - Reproductive biology (medical aspects to be 3)
    10605 - Developmental biology
    10608 - Biochemistry and molecular biology
    10609 - Biochemical research methods
    10610 - Biophysics
    30101 - Human genetics

Completed project evaluation

  • Provider evaluation

    V - Vynikající výsledky projektu (s mezinárodním významem atd.)

  • Project results evaluation

    New chem.modified Hg electrodes and solid amalgam electrodes for parallel analysis of proteins were proposed.Detection and characterization of α-synuclein oligomers unraveled possible initial events in Parkinson´s disease related to oxidative stress

Solution timeline

  • Realization period - beginning

    Jan 1, 2009

  • Realization period - end

    Dec 31, 2011

  • Project status

    U - Finished project

  • Latest support payment

    Mar 18, 2011

Data delivery to CEP

  • Confidentiality

    S - Úplné a pravdivé údaje o projektu nepodléhají ochraně podle zvláštních právních předpisů

  • Data delivery code

    CEP12-AV0-KJ-U/01:1

  • Data delivery date

    May 25, 2012

Finance

  • Total approved costs

    1,620 thou. CZK

  • Public financial support

    1,620 thou. CZK

  • Other public sources

    0 thou. CZK

  • Non public and foreign sources

    0 thou. CZK

Basic information

Recognised costs

1 620 CZK thou.

Public support

1 620 CZK thou.

100%

Provider

Academy of Sciences of the Czech Republic

CEP

BO - Biophysics

Solution period

01. 01. 2009 - 31. 12. 2011

Similar projects(10)

New strategy for inhibition of amyloid fibril formation (GJ18-06255Y) Molecular pathology and genetic diagnostics of Parkinson's disease (NT11331) In-situ structural architecture and cellular interactions of Tau neurofibrils (GN22-15175I)